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Expanded human NK cells armed with CAR uncouple potent anti-tumor activity from off-tumor toxicity against solid tumors

机译:扩展的人NK细胞武装有汽车uncopol uncopory抗肿瘤活性免受实体肿瘤的卵巢毒性

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摘要

Despite the remarkable success of chimeric antigen receptor (CAR)-T cells against hematologic malignancies, severe off-tumor effects have constrained their use against solid tumors. Recently, CAR-engineered natural killer (NK) cells have emerged as an effective and safe alternative. Here, we demonstrate that HER2 CAR-expression in NK cells from healthy donors and patients with breast cancer potently enhances their anti-tumor functions against various HER2-expressing cancer cells, regardless of MHC class I expression. Moreover, HER2 CAR-NK cells exert higher cytotoxicity than donor-matched HER2 CAR-T cells against tumor targets. Importantly, unlike CAR-T cells, HER2 CAR-NK cells do not elicit enhanced cytotoxicity or inflammatory cytokine production against non-malignant human lung epithelial cells with basal HER2 expression. Further, HER2 CAR-NK cells maintain high cytotoxic function in the presence of immunosuppressive factors enriched in solid tumors. These results show that CAR-NK cells may be a highly potent and safe source of immunotherapy in the context of solid tumors.
机译:尽管嵌合抗原受体(汽车)-T细胞对血液学恶性肿瘤的令人显着的成功,但严重的离肿瘤效应已经限制了它们对固体瘤的使用。最近,汽车工程化的天然杀手(NK)细胞已成为有效和安全的替代品。在这里,我们证明HER2在来自健康供体和乳腺癌患者的NK细胞中的轿厢表达效果效果,无论MHC I类表达如何,患者对各种同学癌细胞的抗肿瘤功能。此外,HER2 CAR-NK细胞比供体匹配的HER2的HER2 CAR-T细胞施加更高的细胞毒性,对抗肿瘤靶标。重要的是,与Car-T细胞不同,HER2 Car-NK细胞不引起增强的细胞毒性或炎症细胞因子产生与基础HER2表达的非恶性人肺上皮细胞。此外,HER2 CAR-NK细胞在富含固体瘤中的免疫抑制因子存在下保持高细胞毒性功能。这些结果表明,在实体肿瘤的背景下,汽车NK细胞可能是一种高度有效和安全的免疫疗法来源。

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